Cancer tolerance to chromosomal instability is driven by Stat1 inactivation <i>in vivo</i>

Schubert, Michaël; Hong, Christy; Jilderda, Laura J; Requesens-Rueda, Marta; Tijhuis, Andréa E.; Simon, Judith E; Bakker, Petra L.; Cooper, Jennifer L.; Damaskou, Aristi; Wardenaar, René; Bakker, Björn; Gupta, Sahil; Brink, Anouk van den; Andrade-Ruiz, Lorena; Koster, Mirjam H.; Youssef, Sameh A.; Luinenburg, Daniëlle; Strong, Alex; Engleiter, Thomas; Ponstingl, Hannes; Haan, Gerald de; Bruin, Alain de; Rad, Roland; Nijman, Hans W.; Medema, René H.; Vugt, Marcel A.T.M. van; Bruyn, Marco de; Spierings, Diana C.J.; Colome-Thatche, Maria; Vassiliou, George S.; Foijer, Floris

doi:10.1101/2021.12.03.471107

2021

DOI: 10.1101/2021.12.03.471107

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Cancer tolerance to chromosomal instability is driven by Stat1 inactivation in vivo

Michaël Schubert

Christy Hong

Laura J Jilderda

et al.

Abstract: Chromosomal instability is a hallmark of cancer, but also an instigator of aneuploidy-induced stress, reducing cellular fitness. To better understand how cells with CIN adjust to aneuploidy and adopt a malignant fate in vivo, we performed a genome-wide mutagenesis screen in mice. We find that specifically aneuploid tumors inactivate Stat1 signaling in combination with increased Myc activity. By contrast, loss of p53 is common, but not enriched in CIN tumors. Validation in another tissue type confirmed that CIN… Show more

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Cited by 5 publications

References 77 publications

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Chromosomal instability and inflammation: a catch-22 for cancer cells

2023

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Chromosomal instability (CIN), an increased rate of chromosomal segregation abnormalities, drives intratumor heterogeneity and affects most human cancers. In addition to chromosome copy number alterations, CIN results in chromosome(s) (fragments) being mislocalized into the cytoplasm in the form of micronuclei. Micronuclei can be detected by cGAS, a double-strand nucleic acid sensor, which will lead to the production of the second messenger 2′3′-cGAMP, activation of an inflammatory response, and downstream immune cell activation. However, the molecular network underlying the CIN-induced inflammatory response is still poorly understood. Furthermore, there is emerging evidence that cancers that display CIN circumvent this CIN-induced inflammatory response, and thus immune surveillance. The STAT1, STAT3, and NF-κB signaling cascades appear to play an important role in the CIN-induced inflammatory response. In this review, we discuss how these pathways are involved in signaling CIN in cells and how they are intertwined. A better understanding of how CIN is being signaled in cells and how cancer cells circumvent this is of the utmost importance for better and more selective cancer treatment.

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Chromosomal instability and inflammation: a catch-22 for cancer cells

2023

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Interferon signaling promotes tolerance to chromosomal instability during metastatic evolution in renal cancer

et al. 2023

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Molecular routes to metastatic dissemination are critical determinants of aggressive cancers. Through in vivo CRISPR–Cas9 genome editing, we generated somatic mosaic genetically engineered models that faithfully recapitulate metastatic renal tumors. Disruption of 9p21 locus is an evolutionary driver to systemic disease through the rapid acquisition of complex karyotypes in cancer cells. Cross-species analysis revealed that recurrent patterns of copy number variations, including 21q loss and dysregulation of the interferon pathway, are major drivers of metastatic potential. In vitro and in vivo genomic engineering, leveraging loss-of-function studies, along with a model of partial trisomy of chromosome 21q, demonstrated a dosage-dependent effect of the interferon receptor genes cluster as an adaptive mechanism to deleterious chromosomal instability in metastatic progression. This work provides critical knowledge on drivers of renal cell carcinoma progression and defines the primary role of interferon signaling in constraining the propagation of aneuploid clones in cancer evolution.

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KIF2C/MCAK a prognostic biomarker and its oncogenic potential in malignant progression, and prognosis of cancer patients: a systematic review and meta-analysis as biomarker

Kreis,

Moon,

Wordeman

et al. 2024

Critical Reviews in Clinical Laboratory Sciences

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Cancer tolerance to chromosomal instability is driven by Stat1 inactivation in vivo

Cited by 5 publications

References 77 publications

Chromosomal instability and inflammation: a catch-22 for cancer cells

Chromosomal instability and inflammation: a catch-22 for cancer cells

Interferon signaling promotes tolerance to chromosomal instability during metastatic evolution in renal cancer

KIF2C/MCAK a prognostic biomarker and its oncogenic potential in malignant progression, and prognosis of cancer patients: a systematic review and meta-analysis as biomarker

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